1996
DOI: 10.1016/s0966-3274(96)80016-5
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Chronic rejection of concordant aortic xenografts in the hamster-to-rat model

Abstract: Several groups have demonstrated that it is possible to obtain long-term graft survival of concordant xenografts. One of the important questions that remains is whether xenografts are susceptible to chronic rejection. To answer this question we used the aorta transplantation model. One centimetre of hamster aorta was interposed in the abdominal aorta of Lewis rat recipients. The recipients were either untreated (group 1), or treated with 10 mg/kg cyclosporine (CsA), given intramuscularly three times a week (gr… Show more

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Cited by 10 publications
(3 citation statements)
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“…In all transplants the cellular infiltration was dominated by macrophages, with the T lymphocyte as the next most abundant cell type. Similar findings have been described in several xenogeneic experimental models, vascularized as well as non‐vascularized [3, 4, 13–15].…”
Section: Discussionsupporting
confidence: 87%
“…In all transplants the cellular infiltration was dominated by macrophages, with the T lymphocyte as the next most abundant cell type. Similar findings have been described in several xenogeneic experimental models, vascularized as well as non‐vascularized [3, 4, 13–15].…”
Section: Discussionsupporting
confidence: 87%
“…Aortic transplantation has long been accepted as a relevant small animal model for the investigation of chronic allograft vasculopathy. Scheringa et al [21] used the same model that we have, i.e. hamster aortas transplanted into Lewis rats, and have found neointimal proliferation does take place in his model and that the lesion is inhibited by cyclosporin.…”
Section: Discussionmentioning
confidence: 89%
“…Because intimal proliferation, collagen deposition and SMC proliferation do not occur in this model until 2 weeks after transplantation, chronic rejection features were not found. 28,31 As recently suggested, lymphocyte surface antigen expression reflects the host cellular responsiveness and can thus be used to monitor the pharmacodynamic effects of immunosuppressive agents. 32 A significantly decreased upregulation of CD25 could be demonstrated for FK778 HD and tacrolimus HD and their combination regimen at times of 24-hour trough levels.…”
Section: Discussionmentioning
confidence: 99%